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synergistic effects of pazopanib and hyperthermia against uterine leiomyosarcoma growth mediated by downregulation of histone acetyltransferase 1
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نویسنده
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lin chiao-yun ,chao angel ,wu ren-chin ,lee li-yu ,ueng shir-hwa ,tsai chia-lung ,lee yun-shien ,peng meng-ting ,yang lan-yan ,huang huei-jean ,wang hsin-shih ,lai chyong-huey
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منبع
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journal of molecular medicine - 2020 - دوره : 98 - شماره : 8 - صفحه:1175 -1188
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چکیده
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Pazopanib—a multitargeted tyrosine kinase inhibitor with prominent antiangiogenic effects—has shown promise in the treatment of soft-tissue sarcomas. hyperthermia has been also applied as an adjunctive treatment to chemotherapy for these malignancies. here, we show that pazopanib and hyperthermia act synergistically in inhibiting uterine leiomyosarcoma (lms) cell growth. compared with either treatment alone, the combination of pazopanib and hyperthermia exerted the highest antitumor activity in a xenograft model. mechanistically, we found that combined treatment with pazopanib and hyperthermia inhibited histone acetyltransferase 1 (hat1) expression in lms cells. the clock element on the hat1 promoter was critical for pazopanib- and hyperthermia-induced hat1 downregulation. inhibition of hat1—either by pazopanib and hyperthermia or through hat1 silencing—was mediated by suppression of clock. accordingly, clock protein reconstitution rescued both hat1 levels and hat1-mediated histone acetylation. immunohistochemistry revealed a higher expression of hat1 in uterine lms than in leiomyomas (p = 0.007), with high hat1 expression levels being associated with poor clinical outcomes (p = 0.007). we conclude that pazopanib and hyperthermia exert synergistic effects against lms growth by inhibiting hat1. further preclinical studies on hat1 as a potential drug target in uterine lms are warranted, especially in combination with hyperthermia.
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کلیدواژه
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pazopanib ,hyperthermia ,uterine leiomyosarcoma ,histone acetyltransferase 1 ,clock
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آدرس
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chang gung memorial hospital linkou medical center and chang gung university, college of medicine, department of obstetrics and gynecology, taiwan. chang gung memorial hospital linkou medical center, gynecologic cancer research center, taiwan, chang gung memorial hospital linkou medical center and chang gung university, college of medicine, department of obstetrics and gynecology, taiwan. chang gung memorial hospital linkou medical center, gynecologic cancer research center, taiwan, chang gung memorial hospital linkou medical center and chang gung university, college of medicine, department of anatomic pathology, taiwan, chang gung memorial hospital linkou medical center and chang gung university, college of medicine, department of anatomic pathology, taiwan, chang gung memorial hospital linkou medical center and chang gung university, college of medicine, department of anatomic pathology, taiwan, chang gung memorial hospital linkou medical center, genomic medicine research core laboratory, taiwan, chang gung memorial hospital linkou medical center, genomic medicine research core laboratory, taiwan. ming chuan university, department of biotechnology, taiwan, chang gung memorial hospital linkou medical center and chang gung university, college of medicine, department of medical oncology, taiwan, chang gung memorial hospital linkou medical center, clinical trial center, biostatistics unit, taiwan, chang gung memorial hospital linkou medical center and chang gung university, college of medicine, department of obstetrics and gynecology, taiwan. chang gung memorial hospital linkou medical center, gynecologic cancer research center, taiwan, chang gung memorial hospital linkou medical center and chang gung university, college of medicine, department of obstetrics and gynecology, taiwan, chang gung memorial hospital linkou medical center and chang gung university, college of medicine, department of obstetrics and gynecology, taiwan. chang gung memorial hospital linkou medical center, gynecologic cancer research center, taiwan
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Authors
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